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首页> 外文期刊>Molecular and Cellular Biology >Transformation of NIH 3T3 cells by DNA of the MCF-7 human mammary carcinoma cell line induces expression of an endogenous murine leukemia provirus.
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Transformation of NIH 3T3 cells by DNA of the MCF-7 human mammary carcinoma cell line induces expression of an endogenous murine leukemia provirus.

机译:MCF-7人乳腺癌细胞系DNA转化NIH 3T3细胞可诱导内源性鼠白血病原病毒的表达。

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Previous studies identified two glycoproteins of 86 (gp86) and 72 (gp72) kilodaltons and two nonglycosylated proteins of 70 (p70) and 19 (p19) kilodaltons which were specifically expressed in NIH cells transformed by DNA of the MCF-7 human mammary carcinoma cell line. Pulse-chase experiments and the use of tunicamycin to inhibit glycosylation suggested that gp86, gp72, and p19 were related as precursor products. Characteristics of the four transformation-associated proteins resembled those of murine leukemia virus (MuLV) proteins. Sera raised against disrupted MuLV immunoprecipitated the same four proteins in extracts of NIH(MCF-7) cells and MuLV-infected NIH 3T3 cells. In addition, a monoclonal antibody against MuLV gp70 immunoprecipitated proteins gp86 and gp72, whereas a monoclonal antibody against MuLV p15(E) immunoprecipitated gp86 and p19. These results indicate that proteins gp86, gp72, and p19 expressed in NIH(MCF-7) transformants correspond to MuLV envelope proteins gp80env, gp70, and p15(E), respectively. The transformation-associated protein p70 appears to be a non-envelope MuLV protein, most likely p65gag. Northern blot analysis confirmed that transformation of NIH cells by MCF-7 mammary carcinoma DNA led to the induction of an endogenous MuLV provirus.
机译:先前的研究确定了86(gp86)和72(gp72)千道尔顿的两种糖蛋白以及70(p70)和19(p19)千道尔顿的两种非糖基化蛋白,它们在由MCF-7人乳癌细胞DNA转化的NIH细胞中特异性表达线。脉冲追踪实验和使用衣霉素抑制糖基化表明,gp86,gp72和p19与前体产物有关。四种与转化相关的蛋白质的特征类似于鼠白血病病毒(MuLV)蛋白质的特征。抵抗破坏的MuLV的血清免疫沉淀了NIH(MCF-7)细胞和MuLV感染的NIH 3T3细胞提取物中的相同四种蛋白质。此外,针对MuLV gp70的单克隆抗体会免疫沉淀蛋白gp86和gp72,而针对MuLV p15(E)的单克隆抗体会免疫沉淀gp86和p19。这些结果表明,在NIH(MCF-7)转化子中表达的蛋白gp86,gp72和p19分别对应于MuLV包膜蛋白gp80env,gp70和p15(E)。与转化相关的蛋白p70似乎是非信封MuLV蛋白,很可能是p65gag。 Northern印迹分析证实,MCF-7乳癌DNA对NIH细胞的转化导致了内源性MuLV原病毒的诱导。

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